69; 95% confidence interval, 1.52 to 1.95 (P = 0.033)). On the contrary, it was reported that high expression Akt inhibitor of CLU was related to favorable prognosis in advanced-stage (stage III) serous ovarian cancer [28]. Although our observations were consistent with previously reported ones that s-CLU mediates cisplatin-induced resistance in ovarian cancer [34], CLU expression was found not to be a prognostic factor among patients with advanced-stage (stage III/IV) ovarian cancer in our patient cohort (data not shown).
Moreover, our study showed that s-CLU is well expressed in many ovarian cancer cell lines assayed and resistant ovarian cancer tissues. Additionally, through mechanisms not yet elucidated, as a consequence EPZ015666 chemical structure of acquired resistance, CLU
biosynthesis is altered and up-regulated in ovarian cancer cells. Optimal surgery is a strong prognosticator for advanced-stage ovarian cancer, which was also found in our advanced-stage patient cohort (data not shown), and it is widely accepted that complete cytoreduction is the most important prognostic factor for ovarian cancer. We found that immunohistochemical expression of CLU showed prognostic significance for the patients with early-stage (stage I/II) patients who underwent complete cytoreduction as a primary surgery, whereas histologic subtype and stage are not associated with their survival. Perhaps, the response to front-line chemotherapy might be one of the most important factors for survival among the patients with early-stage disease. Our result suggests that CLU is related
to survival because overexpression of CLU is related to chemoresistance [35, 36]. That is might be because CLU can result in impaired survival for early-stage cases [26]. Alternatively, overexpression of CLU might increase migration and invasion capacity of ovarian cancer cells [27]. To improve the survival of ovarian cancer patients, we need to develop new combination therapy of cytotoxic drugs better than current standard regimen (TX/carboplatin; TC). However, the result from of GOG182 to find superior regimen to TC was negative, indicating that it might be quite difficult to find new useful combination therapy better than TC [37]. Thus, it is necessary to test the efficacy of molecular targeting drugs such as bevacizumab with or without cytotoxic agents, or the new drugs to modulate sensitivity to platinums and/or taxanes for better survival. S-CLU expression had changed upon acquisition of TX-resistance and TX treatment in ovarian cancer cells and tissues. SiRNA or OGX-011 administration caused efficient depletion of CLU mRNA in vitro. Under these conditions, TX stress induced apoptosis more efficiently in CLU-depleted cells most probably because of enhanced growth rate after s-CLU knock-down which makes cells rapidly trapped in the G2/M arrest by TX as a microtubule stabilizing agent.